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发育中的大鼠后脑桥的硫酸软骨素限制前庭神经核神经元的连合投射。

Chondroitin sulfates in the developing rat hindbrain confine commissural projections of vestibular nuclear neurons.

机构信息

Department of Biochemistry, LKS Faculty of Medicine, The University of Hong Kong, Sassoon Road, Hong Kong, China.

出版信息

Neural Dev. 2012 Feb 3;7:6. doi: 10.1186/1749-8104-7-6.

Abstract

BACKGROUND

Establishing correct neuronal circuitry is crucial to proper function of the vertebrate nervous system. The abundance of chondroitin sulfate (CS) proteoglycans in embryonic neural environments suggests that matrix proteoglycans regulate axonal projections when fiber tracts have not yet formed. Among the early-born neurons, the vestibular nucleus (VN) neurons initiate commissural projections soon after generation at E12.5 and reach the contralateral target by E15.5 in the rat hindbrain. We therefore exploited 24-hour cultures (1 day in vitro (DIV)) of the rat embryos and chondroitinase ABC treatment of the hindbrain matrix to reveal the role of CS moieties in axonal initiation and projection in the early hindbrain.

RESULTS

DiI tracing from the VN at E12.5(+1 DIV) showed contralaterally projecting fibers assuming fascicles that hardly reached the midline in the controls. In the enzyme-treated embryos, the majority of fibers were unfasciculated as they crossed the midline at 90°. At E13.5(+1 DIV), the commissural projections formed fascicles and crossed the midline in the controls. Enzyme treatment apparently did not affect the pioneer axons that had advanced as thick fascicles normal to the midline and beyond, towards the contralateral VN. Later projections, however, traversed the enzyme-treated matrix as unfasciculated fibers, deviated from the normal course crossing the midline at various angles and extending beyond the contralateral VN. This suggests that CSs also limit the course of the later projections, which otherwise would be attracted to alternative targets.

CONCLUSIONS

CS moieties in the early hindbrain therefore control the course and fasciculation of axonal projections and the timing of axonal arrival at the target.

摘要

背景

建立正确的神经元连接对于脊椎动物神经系统的正常功能至关重要。软骨素硫酸盐(CS)蛋白聚糖在胚胎神经环境中的丰富含量表明,当纤维束尚未形成时,基质蛋白聚糖可以调节轴突投射。在早期出生的神经元中,前庭神经核(VN)神经元在 E12.5 后不久就开始进行连合投射,并且在大鼠后脑中于 E15.5 到达对侧靶标。因此,我们利用大鼠胚胎的 24 小时培养物(1 天体外培养(DIV))和后脑基质的软骨素酶 ABC 处理来揭示 CS 部分在早期后脑中轴突起始和投射中的作用。

结果

E12.5(+1DIV)时从 VN 进行的 DiI 示踪显示,对侧投射纤维假定在对照组中几乎无法到达中线的束状。在酶处理的胚胎中,由于纤维在 90°处穿过中线,因此大多数纤维未形成束状。在 E13.5(+1DIV)时,连合投射形成束状并在对照组中穿过中线。酶处理显然不会影响已经作为正常中线和中线以外的粗束状向前推进的先驱轴突,朝向对侧 VN。然而,后来的投射穿过未形成束状的纤维穿过酶处理的基质,以各种角度偏离正常轨迹穿过中线,并延伸到对侧 VN 以外。这表明 CS 也限制了后来投射的轨迹,否则这些投射会被吸引到替代靶标。

结论

因此,早期后脑中的 CS 部分控制着轴突投射的轨迹和束状,以及轴突到达靶标的时间。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e7ad/3295737/abac9222b542/1749-8104-7-6-1.jpg

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